首页> 外文期刊>Basic Research in Cardiology >Secretome of apoptotic peripheral blood cells (APOSEC) attenuates microvascular obstruction in a porcine closed chest reperfused acute myocardial infarction model: role of platelet aggregation and vasodilation
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Secretome of apoptotic peripheral blood cells (APOSEC) attenuates microvascular obstruction in a porcine closed chest reperfused acute myocardial infarction model: role of platelet aggregation and vasodilation

机译:凋亡性外周血细胞分泌蛋白组(APOSEC)减轻猪封闭胸腔再灌注急性心肌梗死模型中的微血管阻塞:血小板聚集和血管舒张的作用

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Although epicardial blood flow can be restored by an early intervention in most cases, a lack of adequate reperfusion at the microvascular level is often a limiting prognostic factor of acute myocardial infarction (AMI). Our group has recently found that paracrine factors secreted from apoptotic peripheral blood mononuclear cells (APOSEC) attenuate the extent of myocardial injury. The aim of this study was to determine the influence of APOSEC on microvascular obstruction (MVO) in a porcine AMI model. A single dose of APOSEC was intravenously injected in a closed chest reperfused infarction model. MVO was determined by magnetic resonance imaging and cardiac catheterization. Role of platelet function and vasodilation were monitored by means of ELISA, flow cytometry, aggregometry, western blot and myographic experiments in vitro and in vivo. Treatment of AMI with APOSEC resulted in a significant reduction of MVO. Platelet activation markers were reduced in plasma samples obtained during AMI, suggesting an anti-aggregatory capacity of APOSEC. This finding was confirmed by in vitro tests showing that activation and aggregation of both porcine and human platelets were significantly impaired by co-incubation with APOSEC, paralleled by vasodilator-stimulated phosphoprotein (VASP)-mediated inhibition of platelets. In addition, APOSEC evidenced a significant vasodilatory capacity on coronary arteries via p-eNOS and iNOS activation. Our data give first evidence that APOSEC reduces the extent of MVO during AMI, and suggest that modulation of platelet activation and vasodilation in the initial phase after myocardial infarction contributes to the improved long-term outcome in APOSEC treated animals.
机译:尽管在大多数情况下可以通过早期干预来恢复心外膜血流量,但在微血管水平上缺乏足够的再灌注通常是急性心肌梗死(AMI)的预后因素。我们的小组最近发现,凋亡性外周血单核细胞(APOSEC)分泌的旁分泌因子可减轻心肌损伤的程度。本研究的目的是确定APOSEC对猪AMI模型中微血管阻塞(MVO)的影响。在封闭的胸腔再灌注梗死模型中静脉注射单剂量的APOSEC。通过磁共振成像和心脏导管检查确定MVO。通过ELISA,流式细胞术,凝集测定,蛋白质印迹和体外和体内肌电图实验监测血小板功能和血管舒张作用。用APOSEC治疗AMI可显着降低MVO。 AMI期间获得的血浆样品中的血小板活化标记物减少,表明APOSEC具有抗聚集能力。通过体外试验证实了这一发现,该试验显示,与APOSEC共同孵育会同时破坏猪和人血小板的活化和聚集,同时与血管舒张剂刺激的磷蛋白(VASP)介导的血小板抑制作用平行。此外,APOSEC还通过p-eNOS和iNOS激活证明了冠状动脉具有明显的血管舒张能力。我们的数据提供了第一个证据,即APOSEC可以降低AMI期间MVO的程度,并表明在心肌梗塞后初始阶段,血小板活化和血管舒张的调节有助于改善APOSEC治疗动物的长期预后。

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